Q&A 219.4

What is serotonin syndrome and which medicines cause it?

Prepared by UK Medicines Information (UKMi) pharmacists for NHS healthcare professionals

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Date prepared: 6th December 2016

Background

Serotonin syndrome has been highlighted by the widespread use of serotonergic agents, such as those used to treat depression e.g. selective serotonin reuptake inhibitors (SSRIs) (1). The first reported fatality from serotonin syndrome was over 50 years ago (2), prior to the availability of SSRIs. The incidence of serotonin syndrome is not known but has risenas a result of the increased use of serotonergic drugs and the increasing awareness of this syndrome (3).

Serotonin syndrome can be difficult to differentiate from other medical conditions including, Neuroleptic Malignant Syndrome, anticholinergic toxicity and malignant hyperthermia (3). Healthcare professionals need an awareness of the range of symptoms of serotonin syndrome and drugs with serotonergic activity, which are discussed in this Medicines Q&A. This knowledge will aid early diagnosis and treatment and reduce patient distress as well as potential morbidity and mortality (3).

For in-depth information on specific interactions and switching between medicines see:

UKMi Q&A 48 Triptansand SSRIor SNRI antidepressants – is there an interaction?

UKMi Q&A 94 What is the risk of developing Serotonin Syndrome following concomitant use of tramadol with selective serotonin reuptake inhibitors (SSRIs)?

UKMi QA 150 How do you switch between tricyclic, SSRI and related antidepressants?

UKMi Q&A 151How do you switch between monoamine oxidase inhibitors and SSRI, tricyclic or related antidepressants?

UKMi QA 192 What is the risk of interaction between opioid analgesics and monoamine oxidase inhibitors(MAOIs)?

Answer

The term ‘serotonin syndrome’ is used to describe significant ‘serotonin toxicity’ and the two terms tend to be used interchangeably (1,2). Current thinking favours the spectrum concept of ‘serotonin toxicity’ as a continuum of serotonergic effects. This progresses from side effects through to life-threatening toxicity, with increasing intrasynaptic serotonin levels. Therefore it is a form of poisoning rather than an idiosyncratic reaction (4). It is due to a toxic hyperserotonergic state from hyperstimulation of the brain stem and spinal cord 5HT1A and 5HT2 receptors (5), possibly with more involvement of the latter (1).

The different mechanisms of causing serotonin syndrome are (3):

increase in serotonin synthesis

inhibition of serotonin metabolism

increase in serotonin release

inhibition of serotonin uptake

activation of serotonergic receptors

Serotonin syndrome can occur from:

  1. Overdose of a serotonergic agent e.g. in a case series approximately 15% of patients taking an acute overdose of SSRIs developed moderate serotonin toxicity (1).
  1. Drug interactions i.e. when more than one drug affecting the serotonin system or inhibiting the metabolism of serotonergic drugs istaken (3).
  • For example, serotonin toxicity is a potential danger of administering two serotonergic antidepressants together (6). In cases of serotonin syndrome due to drug interactions, the most severe cases are seen when monoamine oxidase inhibitors (MAOIs), are taken in combination with SSRIs, tricyclic antidepressants or venlafaxine. This is because the mechanism of action of MAOIs is to inhibit the breakdown of serotonin (3,7).
  • Many drugs, in addition to SSRIs, can inhibit the cytochrome P450 2D6 and/or 3A4 isoenzymes, resulting in the accumulation of serotonergic drugs that are being used simultaneously (3).
  1. Taking one serotonergic agent alone in susceptible individuals (8).

A complete and accurate medication history is essential when diagnosing serotonin syndrome (3,8), which usually occurs within a few hours of drug or dose changes, resolving within about 24 hours of stopping the serotonergic drug(s) (5).

Symptoms
Serotonin syndrome or toxicity results in certain symptomsconsisting of a triad of features: alteration of mental status, neuromuscular abnormalities and autonomic hyperactivity (2,3). These three features are not necessarily present together in every patient (7). Clinical features can range from mild to life-threatening (3). Around 40% of patients have mental status changes, about 50% of patients have evidence of neuromuscular hyperactivity. Autonomic instability occurs in around 40% of patients (7). Severe cases may result in complications, such as seizures, rhabdomyolysis, myoglobinuria, metabolic acidosis, renal failure, acute respiratory distress syndrome, respiratory failure, diffuse intravascular clotting, coma, and death (3).

Table 1. Symptoms of Serotonin Syndrome (3)

Alteration of mental status / Neuromuscular abnormalities / Autonomic hyperactivity
agitation / tremors / hypertension
anxiety / clonus / tachycardia
disorientation / hyperreflexia / tachypnea
restlessness / muscle rigidity / hyperthermia
excitement / bilateral babinski signs / mydriasis
diaphoresis
dry mucous membranes
flushed skin
shivering
vomiting
diarrhoea
hyperactive bowel sounds
arrhythmias

Several systems of diagnostic criteria exist, for example the Sternbach criteria and the Hunter Serotonin Toxicity Criteria (HSTC). The HSTCare the most accurate and specific criteria and areless likely to miss early, mild or subacute forms of serotonin syndrome (8).

Hunter serotonin toxicity criteria – in the presence of a serotonergic agent plus one of the following (3,8):

Spontaneous clonus

Inducible or ocular clonus AND agitation or diaphoresis

Tremor AND hyperreflexia

Hypertonia AND hyperpyrexia (temperature exceeding 38ºC) AND ocular orinducible clonus

Causative medicines

Serotonin syndrome can be caused by certain drugs alone (usually in overdose) or combinations of serotonergic drugs (8). Clinicians should be aware of drugs that have serotonergic effects and the combination of any two should therefore be used sparingly or with great caution (3). Some of these medicines are in therapeutic groups that would not normally be associated with use in depression, or psychiatry in general, so their serotonergic effects are not immediately apparent (1). These include drugs such as linezolid or selegiline, both of which have MAOI activity (3). See Table 2 below for further examples.

Life-threatening cases of serotonin syndrome may occur, for example with the use of any MAOI (e.g. phenelzine, tranylcypromine) in combination with SSRIs (1). Washout periods should be observed when switching between these antidepressants. See UKMi Q&A151 How do you switch between monoamine oxidase inhibitors and SSRI, tricyclic or related antidepressants? for further details on switching from an SSRI to an MAOI and vice versa.

Table 2. Examples of medicines with potential to cause serotonin syndrome (1,3,5,8-10)

This list (see limitations below) only includes examples of medicines with serotonergic effects. Examples of medicines which have the potential to cause serotonin syndrome solely via cytochrome P450 interactions have been excluded.

Therapeutic group / Examples of medicines
SSRI antidepressants / Citalopram, escitalopram, fluoxetine, fluvoxamine, paroxetine, sertraline
SNRI antidepressants / Venlafaxine, duloxetine
MAOI antidepressants / Tranylcypromine, phenelzine, moclobemide (reversible MAO-A inhibitor), isocarboxazid
Tricyclic antidepressants / Clomipramine, imipramine, amitriptyline, doxepin, nortriptyline, trimipramine
Miscellaneous / Lithium, trazodone, L-tryptophan, mirtazapine, dapoxetine, vortioxetine
Opioids / Pethidine, tramadol, methadone, fentanyl, dextromethorphan, pentazocine, oxycodone, tapentadol
Parkinson’s disease treatment / Selegiline (MAO-B inhibitor), rasagiline (MAO-B inhibitor), levodopa, amantadine, safinamide
Antibacterials / Linezolid, tedizolid (reversible MAOI activity (11))
Anti-cancer drugs / Procarbazine
Anticonvulsants / Carbamazepine, valproate
Antiemetics / Metoclopramide, ondansetron, granisetron
Antihistamines / Chlorphenamine, diphenhydramine
Antimigraine drugs / Triptans (See UKMi QA48) e.g. frovatriptan, almotriptan, eletriptan, naratriptan, rizatriptan, sumatriptan, zolmitriptan. Dihydroergotamine.
Anti-smoking aids / Bupropion
Anxiolytics / Buspirone
Diagnostic dye / Methylthioninium chloride (methylene blue) (12) - has MAOI activity(3)
Herbal products / St John’s wort

Summary

The spectrum of ‘serotonin toxicity’ relates to a form of poisoning, not an idiosyncratic reaction. It progresses from mild to life-threatening toxicity, with increasing intrasynaptic serotonin levels (4).

Serotonin syndrome is due to a toxic hyperserotonergic state from hyperstimulation of the brain stem and spinal cord 5HT1A and 5HT2 receptors (5), possibly with more involvement of the latter (1).

Serotonin syndrome can occur from an overdose, drug interaction or even single drug therapy in susceptible individuals with a serotonergic agent (1,3,8).

Symptoms consist of alteration of mental status, neuromuscular abnormalities and autonomic hyperactivity (2,3). Patients do not necessarily have all three features (7).

Medicines potentially causing serotonin syndrome all have some form of serotonergic activity (1).

Limitations

Information on the treatment of serotonin syndrome is beyond the scope of this Medicines Q&A.
This Medicines Q&A includes key examples only of medicines available in the UK with the potential to cause serotonin syndrome – the list in Table 2 is not exhaustive. This list also only includes examples of medicines with serotonergic effects. Examples of medicines which have the potential to cause serotonin syndrome solely via cytochrome P450 interactions have been excluded. It does not encompass amphetamine and its derivative drugs of misuse, which are also known to cause serotonin syndrome.

This Medicines Q&A is based on key review papers i.e. not single case reports.

References

  1. Buckley NA, Dawson AH, Isbister GK. Serotonin syndrome. BMJ 2014: 348:g1626.
  2. Gillman K, Whyte IM. Serotonin syndrome. Chapter 3 in Haddad P, Dursun S, Deakin B,editors. Adverse Syndromes and Psychiatric Drugs: a Clinical Guide. Oxford: Oxford University Press; 2005 p 37-49.
  3. Volpi-Abadie J, Kaye AM, Kaye AD. Serotonin syndrome. The Ochsner Journal 2013: 13: 533-540.
  4. Gillman PK. A Review of Serotonin Toxicity Data: Implications for the Mechanisms of Antidepressant Drug Action. Biol Psychiatry 2006; 59: 1046-1051.
  5. Bazire S. Psychotropic Drug Directory: The Professionals’ Pocket Handbook and Aide Memoire. Lloyd-Reinhold Publications UK; 2016 p490
  6. Taylor D, Paton C, Kapur S. The Maudsley Prescribing Guidelines 12th Edition.Chichester: John Wiley and Sons, Ltd 2015 p296.
  7. Thanacoody R. Serotonin syndrome. Medicine 2007;35(10):556-557.
  8. Boyer EW. Serotonin syndrome. In: UpToDate. Wolters Kluwer Health.Last updated 2nd July 2014. Accessed via on 6thDecember 2016
  9. Boyer EW, Shannon M. The Serotonin Syndrome. N Engl J Med 2005; 352(11):1112-20.
  10. Preston CL (ed),Stockley’s Drug Interactions. [online] London: Pharmaceutical Press < (accessed on6th December 2016).
  11. Joint Formulary Committee.British National Formulary(online) London: BMJ Group and Pharmaceutical Press < [Accessed on 6th December 2016]
  12. Medicines and Healthcare products Regulatory Agency. Methylthioninium chloride (methylene blue): Update on CNS toxicity with serotonergic drugs. Drug Safety Update April 2009; 2(9):3.

Quality Assurance

Prepared by

Joshua McKie, Lead Pharmacist Critical Evaluation, (based on earlier work by Marc Miell, Sandra Hicks and Kate Pickett), Southampton Medicines Advice Service, University Hospital Southampton NHS Foundation Trust.

Date Prepared

6th December 2016

Checked by
Samantha Owen, Principal Pharmacist Critical Evaluation, Southampton Medicines Advice Service, University Hospital Southampton NHS Foundation Trust.

Date of check

9th December 2016

Search strategy

  • Embase (via OVID): exp SEROTONIN SYNDROME/ [Limit to: Publication Year 2014-current and (Publication Types Review) and Human and English Language]
  • Medline (via OVID): exp SEROTONIN SYNDROME/ [Limit to: Publication Year 2014-Current, Review Articles and English Language].
  • NICEEvidence. Accessed via
  • In-house textbooks

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Available throughNICE Evidence Search at